TLR2 engagement on CD4 super(+) T cells enhances effector functions and protective responses to Mycobacterium tuberculosis

We have previously demonstrated that mycobacterial lipoproteins engage TLR2 on human CD4 super(+) T cells and upregulate TCR-triggered IFN-[gamma] secretion and cell proliferation in vitro. Here we examined the role of CD4 super(+) T-cell-expressed TLR2 in Mycobacterium tuberculosis (MTB) Ag-specific T-cell priming and in protection against MTB infection in vivo. Like their human counterparts, mouse CD4 super(+) T cells express TLR2 and respond to TLR2 costimulation in vitro. This Th1-like response was observed in the context of both polyclonal and Ag-specific TCR stimulation. To evaluate the role of T-cell TLR2 in priming of CD4 super(+) T cells in vivo, naive MTB Ag85B-specific TCR transgenic CD4 super(+) T cells (P25 TCR-Tg) were adoptively transferred into Tlr2 super(-/-) recipient C57BL/6 mice that were then immunized with Ag85B and with or without TLR2 ligand Pam sub(3)Cys-SKKKK. TLR2 engagement during priming resulted in increased numbers of IFN-[gamma]-secreting P25 TCR-Tg T cells 1 week after immunization. P25 TCR-Tg T cells stimulated in vitro via TCR and TLR2 conferred more protection than T cells stimulated via TCR alone when adoptively transferred before MTB infection. Our findings indicate that TLR2 engagement on CD4 super(+) T cells increases MTB Ag-specific responses and may contribute to protection against MTB infection.